Dulaglutide: Difference between revisions

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| generic = Dulaglutide

| brand = Trulicity

| structure = '''Fc-fusion construct''': two identical GLP-1 analog peptides (each modified at positions 8, 22, 36 for DPP-4 resistance and reduced immunogenicity) linked to a human IgG4 Fc fragment via a small glycine-rich peptide linker. The Fc tail drives the long half-life through FcRn recycling.<ref name="glaesner2010">Glaesner W, Vick AM, Millican R et al. (2010). Engineering and characterization of the long-acting glucagon-like peptide-1 analogue LY2189265, an Fc fusion protein. ''Diabetes Metab Res Rev'' 26(4):287–96. doi:10.1002/dmrr.1080</ref>

| structure =

| classes = [[GLP-1 receptor agonist]] · [[Antidiabetic medicines|Antidiabetic]] · Fc-fusion biologic

| mechanism = ~~Selective long~~-acting agonist of the [[GLP-1 receptor]]~~. The~~ Fc-~~IgG4 structure differentiates it pharmacokinetically (large protein cleared by FcRn-mediated recycling rather than albumin binding) but the receptor pharmacology is the standard GLP-1 RA profile~~.~~<ref name="glaesner2010"/>~~

| mechanism = Long-acting agonist of the [[GLP-1 receptor]]; Fc-fusion construct.

| uses = [[Type 2 diabetes mellitus]] · [[Cardiovascular risk reduction]] in T2DM

| starting_dose = 0.75 mg SC weekly<ref name="trulicity-label">US FDA. ''Trulicity (dulaglutide) prescribing information.'' Eli Lilly. https://www.accessdata.fda.gov/drugsatfda_docs/label/2022/125469s044lbl.pdf</ref>

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| pregnancy = Avoid. Discontinue at least 1 month before planned pregnancy. Animal data show embryofetal harm.<ref name="trulicity-label"/>

| legal = Rx-only;<ref name="trulicity-label"/> not a controlled substance

| intro = Dulaglutide is a weekly subcutaneous [[GLP-1 receptor agonist]] developed by Eli Lilly, marketed as '''[[Trulicity]]''' since September 2014.<ref name="trulicity-label"/> Structurally distinct from the acylated peptide GLP-1 RAs ([[semaglutide]], [[liraglutide]]), dulaglutide is an Fc-fusion biologic — its long half-life comes from FcRn-mediated recycling rather than albumin binding.<ref name="glaesner2010"/>

| intro = Dulaglutide is a weekly subcutaneous [[GLP-1 receptor agonist]] developed by Eli Lilly, marketed as '''[[Trulicity]]''' since September 2014.<ref name="trulicity-label"/> Structurally distinct from the acylated peptide GLP-1 RAs ([[semaglutide]], [[liraglutide]]), dulaglutide is an Fc-fusion biologic, its long half-life comes from FcRn-mediated recycling rather than albumin binding.<ref name="glaesner2010"/>

Dulaglutide's principal clinical distinction is the [[REWIND trial|REWIND trial]], in which dulaglutide reduced major adverse cardiovascular events by 12% in T2DM patients ''including a majority with no prior cardiovascular disease'', making it the first GLP-1 RA to demonstrate cardiovascular benefit in ''primary'' prevention.<ref name="rewind">Gerstein HC et al. (2019). Dulaglutide and cardiovascular outcomes in type 2 diabetes (REWIND). ''Lancet'' 394(10193):121–30. doi:10.1016/S0140-6736(19)31149-3</ref>

| pharmacokinetics = '''Chemistry'''. '''Fc-fusion construct''': two identical GLP-1 analog peptides (each modified at positions 8, 22, 36 for DPP-4 resistance and reduced immunogenicity) linked to a human IgG4 Fc fragment via a small glycine-rich peptide linker. The Fc tail drives the long half-life through FcRn recycling.<ref name="glaesner2010">Glaesner W, Vick AM, Millican R et al. (2010). Engineering and characterization of the long-acting glucagon-like peptide-1 analogue LY2189265, an Fc fusion protein. ''Diabetes Metab Res Rev'' 26(4):287–96. doi:10.1002/dmrr.1080</ref>

~~Dulaglutide's principal clinical distinction is~~ the ~~[[REWIND trial|REWIND trial]]~~, ~~in which dulaglutide reduced major adverse cardiovascular events by 12% in T2DM patients ''including~~ a ~~majority with no prior cardiovascular disease'' — making it the first GLP~~-~~1 RA to demonstrate cardiovascular benefit in ''primary'' prevention~~.<ref name="~~rewind~~">~~Gerstein HC et al~~. ~~(2019)~~. ~~Dulaglutide and cardiovascular outcomes in type 2 diabetes (REWIND). ''Lancet'' 394(10193):121–30. doi:10.1016/S0140~~-~~6736(19)31149-3<~~/~~ref~~>

The Fc-IgG4 fusion confers protection from renal filtration (~63 kDa, well above the glomerular cutoff) and triggers FcRn-mediated recycling, producing a terminal half-life of ~120 hours.<ref name="glaesner2010"/><ref name="trulicity-label"/> Cleared by proteolytic catabolism; no CYP-mediated metabolism. No dose adjustment for renal or hepatic impairment.<ref name="trulicity-label"/>

~~| pharmacokinetics =~~ The Fc-~~IgG4 fusion confers protection from renal filtration (~63 kDa, well above the glomerular cutoff)~~ and ~~triggers FcRn-mediated recycling~~, ~~producing a terminal half-life of ~120 hours.<ref name="glaesner2010"/><ref name="trulicity-label"/> Cleared by proteolytic catabolism; no CYP-mediated metabolism. No dose adjustment~~ for ~~renal or hepatic impairment~~.~~<ref name="trulicity-label"/>~~

The large molecular size limits both injection-site dispersion and oral bioavailability, dulaglutide cannot be formulated for oral use.

The large ~~molecular size limits both injection~~-~~site dispersion and oral bioavailability — dulaglutide cannot be formulated for oral use~~.

| pharmacodynamics = '''Receptor pharmacology'''. Selective long-acting agonist of the [[GLP-1 receptor]]. The Fc-IgG4 structure differentiates it pharmacokinetically (large protein cleared by FcRn-mediated recycling rather than albumin binding) but the receptor pharmacology is the standard GLP-1 RA profile.<ref name="glaesner2010"/>

~~| pharmacodynamics =~~ At maintenance doses:

At maintenance doses:

* HbA1c reduction of ~0.8–1.5 percentage points (1.5 mg/wk) and ~1.6–1.9 (4.5 mg/wk) in T2DM<ref name="award11">Frias JP, Bonora E, Nevarez Ruiz L et al. (2021). Efficacy and safety of dulaglutide 3 and 4.5 mg versus 1.5 mg in metformin-treated patients with type 2 diabetes (AWARD-11). ''Diabetes Care'' 44(3):765–73. doi:10.2337/dc20-1473</ref>

* Weight loss of ~2–5 kg, dose-dependent<ref name="award11"/>

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* Modest SBP reduction (~1–2 mmHg)<ref name="trulicity-label"/>

| indications = <~~indication~~ ref="diabetes-type-2" author="MDElliottMD"/>

| indications = <problem ref="diabetes-type-2" author="MDElliottMD"/>

<~~indication~~ ref="cv-risk-t2dm" author="MDElliottMD"/>

| dosing = <titration slug="trulicity-standard" author="MDElliottMD" title="Trulicity — standard T2DM titration">

| dosing = <titration slug="trulicity-standard" author="MDElliottMD" title="Trulicity, standard T2DM titration">

0.75 mg SC weekly (starting and minimum effective dose)

→ 1.5 mg SC weekly × ≥4 weeks (most common maintenance)

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| effects = * '''Early satiety''' (less pronounced than with semaglutide/tirzepatide at equipotent HbA1c reduction){{Citation needed}}

* '''Nausea''' — usually mild-to-moderate, peaks in first 2–4 weeks<ref name="trulicity-label"/>

* '''Nausea''', usually mild-to-moderate, peaks in first 2–4 weeks<ref name="trulicity-label"/>

* '''Diarrhea / constipation'''<ref name="trulicity-label"/>

* '''Abdominal pain'''<ref name="trulicity-label"/>

* '''Decreased appetite'''<ref name="trulicity-label"/>

* '''Injection-site reactions''' — uncommon, generally mild<ref name="trulicity-label"/>

* '''Injection-site reactions''', uncommon, generally mild<ref name="trulicity-label"/>

GI tolerability is generally considered modestly better than weekly exenatide and comparable to or slightly better than weekly semaglutide at equivalent glycemic effect.{{Citation needed}}

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| interactions = <pharmaInteractions/>

| pregnancy_details = Avoid. Animal embryofetal toxicity is documented.<ref name="trulicity-label"/> Discontinue at least 1 month before planned conception due to the ~5-day half-life. The pen contains no preservatives — single-dose only.

| pregnancy_details = Avoid. Animal embryofetal toxicity is documented.<ref name="trulicity-label"/> Discontinue at least 1 month before planned conception due to the ~5-day half-life. The pen contains no preservatives, single-dose only.

| monitoring = * Baseline: HbA1c, weight, BP, renal function, lipid panel

* Personal or family history of MTC or [[MEN2]] — '''contraindicated''', do not start<ref name="trulicity-label"/>

* Personal or family history of MTC or [[MEN2]], '''contraindicated''', do not start<ref name="trulicity-label"/>

* Every 3 months for first year: HbA1c, weight, GI tolerability, signs of [[pancreatitis]] or [[gallbladder disease]]

* Annual: renal function, lipids

* '''Pre-procedure''': hold weekly dose ≥7 days before any planned anesthesia<ref name="kindel2024">Kindel TL et al. (2024). Perioperative GLP-1 receptor agonist safety guidance. ''Surg Obes Relat Dis'' 20(12):1183–8.</ref>

| counseling = * Use the pre-filled pen as directed; the needle is hidden — patients do not see it. This is often the preferred GLP-1 RA for needle-averse patients.{{Citation needed}}

| counseling = * Use the pre-filled pen as directed; the needle is hidden, patients do not see it. This is often the preferred GLP-1 RA for needle-averse patients.{{Citation needed}}

* GI side effects peak in first 2–4 weeks, then attenuate.<ref name="trulicity-label"/>

* If a weekly dose is missed: take within 3 days; if >3 days, skip and resume on the next regular day.<ref name="trulicity-label"/>

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}}

~~[[Category:MedCategory]]~~

[[Category:GLP-1 receptor agonists]]

[[Category:Antidiabetic medicines]]

[[Category:Eli Lilly medicines]]

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